Пневмокандин B ₀

Пневмокандин B ₀
Имена
	Имя IUPAC N -{(2 r , 6 с , 9 с , 11 r , 12 r , 14a s , 15 с , 20 с , 23 с , 25a s ) -20-[(1 с ) -3-амино-1-гидрокси -3-оксопропил] -2 3 -[(1 с , 2 с ) -1,2-дигидрокси-2- (4-гидроксифенил) этил] -2,11,12,15-тетрагидрокси-6-[(1 с ) -1-гидроксиэтил] -5,8,14,19,22,25-гексаксоксотетракосагидро-1 H -дипирроло [2,1-C: 2 ', 1'-L] [1,4,7,10,13 , 16] HexaazacyClohenicosin-9-IL} -10,12-диметилтетрадеканамид
	Other names CHEMBL269311; 135575-42-7; Pneumocandin B0; Hydroxy Echinocandin; SCHEMBL8444763
Identifiers
CAS Number	135575-42-7 ;
3D model (JSmol)	Interactive image;
ChEMBL	ChEMBL269311;
ChemSpider	17276932;
ECHA InfoCard	100.157.925
PubChem CID	5742645;
UNII	BA795CZ3I2 ;
	показывать InChI
	показывать SMILES
Properties
Chemical formula	C50H80N8O17
Molar mass	1065.229 g·mol−1
Appearance	White crystalline powder
Density	1.411 g.cm−3
Solubility in water	Soluble in ethanol, methanol, DMF or DMSO. Limited water solubility.
Refractive index (nD)	1.629
	Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa). Infobox references

Пневмокандин B ₀ , также известный как пневмокандин B0 , пневмокандин B (0) и гидрокси эхинокандин , является органическим химическим соединением с формулой C ₅₀ H ₈₀ N ₈ O ₁₇ , ^{[ 1 ]} Производится грибом Glarea lozoyensis .

Это сильный противогрибковое средство и ингибирует синтез β- (1 → 3) -D -гукан, который является фундаментальным компонентом в большинстве клеточных стен , таких как мембрана Candida albicans . Это очень важное занятие, поскольку наблюдается увеличение частоты грибковых инфекций, что сопровождается увеличением разнообразия оппортунистических и патогенных грибов, таких как Candida .

Это соединение используется для синтеза Caspofungin . ^{[ 2 ]}

Пневмокандин B ₀ можно легко спутать с пневмокандином B, хотя они имеют разные боковые цепочки и остатки .

Производство

Pneumocandin B₀ is the starting molecule for the first semisynthetic echinocandin antifungal drug, caspofungin acetate.^{[citation needed]}

In the wild-type strain, pneumocandin B₀ is a minor fermentation product, and its industrial production was achieved by a combination of extensive mutation and medium optimization.^{[citation needed]}

The pneumocandin biosynthetic gene cluster was previously elucidated by a whole genome sequencing approach. Knowledge of the biosynthetic cluster suggested an alternative way to exclusively produce pneumocandin B₀.^{[citation needed]}

Disruption of GLOXY4, encoding a nonheme, α-ketoglutarate-dependent oxygenase, confirmed its involvement in L-leucine cyclization to form (4S)-methyl-L-proline. The absence of (4S)-methyl-L-proline abolishes pneumocandin A₀ production, and (3S)-hydroxyl-L-proline occupies the hexapeptide core's position 6, resulting in exclusive production of pneumocandin B₀.^{[citation needed]}

Retrospective analysis of the GLOXY4 gene in a previously isolated pneumocandin B₀-exclusive mutant (ATCC 74030) indicated that chemical mutagenesis disrupted the GLOXY4 gene function by introducing two amino acid mutations in GLOXY4.^{[citation needed]}

This one-step genetic manipulation can rationally engineer a high-yield production strain.^[3]

Special features

The echinocandins and pneumocandins are lipopeptides antifungal agents that inhibit the synthesis of β-(1→3)-D-glucan, an essential cell wall homopolysaccharide found in many pathogenic fungi.^{[citation needed]}

Compounds with this fungal-specific target have several attractive features:

Lack of mechanism-based toxicity
Potential for fungicidal activity
Activity against strains with intrinsic or acquired resistance mechanisms for existing antimycotics.^[4]

Caspofungin

Caspofungin, a semisynthetic derivate of the pneumocandin B₀, is the first licensed compound of a new class of antifungal agent, that are called the echinocandins. This antifungal agent attacks the fungal cell by selective inhibition of β-(1→3)-D-glucan synthase, which is not present in mammalian cells. Caspofungin represents an interesting and clinically valuable new antifungal drug that broadens the available therapeutic armamentarium for the treatment of invasive fungal infections. ^[5]

Semisynthetic derivatives

The antipneumocystis activities of the pneumocandins can be significantly improved through synthetic modification.

There are new semisynthetic pneumocandin B₀ derivatives that have been found:

By the addition of an aminoethyl ether at the R³ position of pneumocandin B₀ resulted water-soluble and nonprodrug compounds, substantially more efficacious
By the modification of pneumocandin B₀ at the R² position by the conversion of the hydroxyglutamine to a hydroxyornithine increases the antipneumocystis activities of the compounds by 4-fold.

These two modifications combined were synergistic, resulting in a 10-fold improvement in potency against Pneumocystis jirovecii (formerly known as Pneumocystis carinii) pneumonia.^[6]

References

^ "Pneumocandin Bo". Pubchem Open Chemistry Database. Retrieved 17 October 2015.
^ Bouffard, FA; Zambias, RA; Dropinski, JF; Balkovec, JM; Hammond, ML; Abruzzo, GK; Bartizal, KF; Marrinan, JA; Kurtz, MB (21 January 1994). "Synthesis and Antifungal Activity of Novel Cationic Pneumocandin Bo Derivatives". Journal of Medicinal Chemistry. 37 (2): 222–5. doi:10.1021/jm00028a003. PMID 8295208.
^ Chen, Li; Yue, Qun; Li, Yan; Niu, Xuemei; Xiang, Meichun; Wang, Wenzhao; Bills, Gerald F.; Liu, Xingzhong; An, Zhiqiang (2015-03-01). "Engineering of Glarea lozoyensis for Exclusive Production of the Pneumocandin B0 Precursor of the Antifungal Drug Caspofungin Acetate". Applied and Environmental Microbiology. 81 (5): 1550–1558. Bibcode:2015ApEnM..81.1550C. doi:10.1128/AEM.03256-14. ISSN 0099-2240. PMC 4325176. PMID 25527531.
^ Kurtz, M. B.; Douglas, C. M. (1997-01-01). "Lipopeptide inhibitors of fungal glucan synthase". Journal of Medical and Veterinary Mycology. 35 (2): 79–86. doi:10.1080/02681219780000961. ISSN 0268-1218. PMID 9147267.
^ Maschmeyer, Georg; Glasmacher, Axel (2005-07-01). "Pharmacological properties and clinical efficacy of a recently licensed systemic antifungal, caspofungin". Mycoses. 48 (4): 227–234. doi:10.1111/j.1439-0507.2005.01131.x. ISSN 1439-0507. PMID 15982202. S2CID 23214228.
^ Schmatz, DM; Powles, MA; McFadden, D; Nollstadt, K; Bouffard, FA; Dropinski, JF; Liberator, P; Andersen, J (1995). "New Semisynthetic Pneumocandins with Improved Efficacies against Pneumocystis carinii in the Rat". Antimicrob Agents Chemother. 39 (6): 1320–3. doi:10.1128/aac.39.6.1320. PMC 162734. PMID 7574523.

External links

Chemical Book listing

[1] "Pneumocandin Bo". Pubchem Open Chemistry Database. Retrieved 17 October 2015.

[2] Bouffard, FA; Zambias, RA; Dropinski, JF; Balkovec, JM; Hammond, ML; Abruzzo, GK; Bartizal, KF; Marrinan, JA; Kurtz, MB (21 January 1994). "Synthesis and Antifungal Activity of Novel Cationic Pneumocandin Bo Derivatives". Journal of Medicinal Chemistry. 37 (2): 222–5. doi:10.1021/jm00028a003. PMID 8295208.

[3] Chen, Li; Yue, Qun; Li, Yan; Niu, Xuemei; Xiang, Meichun; Wang, Wenzhao; Bills, Gerald F.; Liu, Xingzhong; An, Zhiqiang (2015-03-01). "Engineering of Glarea lozoyensis for Exclusive Production of the Pneumocandin B0 Precursor of the Antifungal Drug Caspofungin Acetate". Applied and Environmental Microbiology. 81 (5): 1550–1558. Bibcode:2015ApEnM..81.1550C. doi:10.1128/AEM.03256-14. ISSN 0099-2240. PMC 4325176. PMID 25527531.

[4] Kurtz, M. B.; Douglas, C. M. (1997-01-01). "Lipopeptide inhibitors of fungal glucan synthase". Journal of Medical and Veterinary Mycology. 35 (2): 79–86. doi:10.1080/02681219780000961. ISSN 0268-1218. PMID 9147267.

[5] Maschmeyer, Georg; Glasmacher, Axel (2005-07-01). "Pharmacological properties and clinical efficacy of a recently licensed systemic antifungal, caspofungin". Mycoses. 48 (4): 227–234. doi:10.1111/j.1439-0507.2005.01131.x. ISSN 1439-0507. PMID 15982202. S2CID 23214228.

[6] Schmatz, DM; Powles, MA; McFadden, D; Nollstadt, K; Bouffard, FA; Dropinski, JF; Liberator, P; Andersen, J (1995). "New Semisynthetic Pneumocandins with Improved Efficacies against Pneumocystis carinii in the Rat". Antimicrob Agents Chemother. 39 (6): 1320–3. doi:10.1128/aac.39.6.1320. PMC 162734. PMID 7574523.

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